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β-乳球蛋白二肽和β-酪蛋白吗啡-7及其代谢产物的体外转运与饱腹感

In vitro transport and satiety of a beta-lactoglobulin dipeptide and beta-casomorphin-7 and its metabolites.

作者信息

Osborne Simone, Chen Wei, Addepalli Rama, Colgrave Michelle, Singh Tanoj, Tran Cuong, Day Li

机构信息

CSIRO Animal, Food and Health Sciences, 306 Carmody Road, St Lucia, QLD 4067, Australia.

出版信息

Food Funct. 2014 Nov;5(11):2706-18. doi: 10.1039/c4fo00164h.

Abstract

Understanding the digestive behaviour and biological activities of dairy proteins may help to develop model dairy products with targeted health outcomes including increased satiety and healthy weight maintenance. Caseins and whey proteins constitute over 95% of milk proteins with consumption of these proteins associated with increased satiety and a decreased prevalence of metabolic disorders. To investigate the in vitro digestive behaviour and satiety of dairy proteins at the intestinal epithelium, the in vitro transport and hydrolysis of 500-2000 μM β-casomorphin-7 (YPFPGPI or β-CM7) and a β-lactoglobulin (β-Lg) dipeptide (YL) was measured using Caco-2 cell monolayers grown on transwells as a model of the intestinal epithelium. Transport of YL was concentration dependent and ranged from 0.37-5.26 × 10(-6) cm s(-1), whereas transport of β-CM7 was only detected at 2000 μM and was significantly lower at 0.13 × 10(-6) cm s(-1). Rapid hydrolysis of β-CM7 in the apical chamber by the Caco-2 cells produced three peptide metabolites: YP, GPI and FPGPI. All of these metabolites were detected in the basolateral chamber after 30 min with both the YP and GPI peptides transporting at a higher rate than intact β-CM7. In vitro satiety was indicated by the secretion of cholecystokinin [26-33] (CCK-8) and glucagon-like peptide 1 (GLP-17-36NH2) in the STC-1 enteroendocrine cell model. CCK-8 secretion was highest in response to β-CM7 followed by the β-CM7 metabolite FPGPI. CCK-8 secretion however was not significantly stimulated by the tri- or dipeptides. Secretion of GLP-1 was not significantly stimulated by β-CM7 or YL. These in vitro results suggest that dairy peptide size enhances CCK-8 secretion, whilst limiting transport across Caco-2 monolayers.

摘要

了解乳蛋白的消化行为和生物活性可能有助于开发具有特定健康功效的模拟乳制品,这些功效包括增强饱腹感和维持健康体重。酪蛋白和乳清蛋白占牛奶蛋白的95%以上,摄入这些蛋白质与饱腹感增强和代谢紊乱患病率降低有关。为了研究乳蛋白在肠上皮细胞中的体外消化行为和饱腹感,使用生长在Transwell上的Caco-2细胞单层作为肠上皮细胞模型,测量了500-2000μMβ-酪蛋白吗啡-7(YPFPGPI或β-CM7)和一种β-乳球蛋白(β-Lg)二肽(YL)的体外转运和水解。YL的转运呈浓度依赖性,范围为0.37-5.26×10(-6) cm s(-1),而β-CM7的转运仅在2000μM时被检测到,且显著低于0.13×10(-6) cm s(-1)。Caco-2细胞在顶室中对β-CM7的快速水解产生了三种肽代谢产物:YP、GPI和FPGPI。30分钟后,所有这些代谢产物在基底外侧室中均被检测到,其中YP和GPI肽的转运速率高于完整的β-CM7。在STC-1肠内分泌细胞模型中,胆囊收缩素[26-33](CCK-8)和胰高血糖素样肽1(GLP-1 7-36NH2)的分泌表明了体外饱腹感。对β-CM7的反应中CCK-8分泌最高,其次是β-CM7代谢产物FPGPI。然而,三肽或二肽并未显著刺激CCK-8分泌。β-CM7或YL并未显著刺激GLP-1的分泌。这些体外研究结果表明,乳肽的大小会增强CCK-8分泌,同时限制其穿过Caco-2单层细胞的转运。

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